Systematic study of substance P analogs. II. Rapid screening of 512 substance P stereoisomers for binding to NK1 receptor.

J X Wang, A J Dipasquale, A M Bray, N J Maeji, D C Spellmeyer, H M Geysen
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Abstract

Recent developments in multiple peptide synthesis have made it feasible to synthesize and screen large numbers of peptide analogs simultaneously. We report here a model study of large scale screening of stereoisomers of substance P with systematic D-amino acid replacements. Such studies are useful in exploring conformational requirements of peptide-receptor interaction and to provide empirical information for peptide drug design. 512 stereoisomers of SP were prepared by the multipin peptide synthesis method. Receptor binding affinities of these analogs were estimated by an iterative competition assay. Results obtained form a comprehensive database on the stereochemical requirement of SP binding to central NK1 receptor. Data from analogs with single D-amino acid replacement are consistent with those previously reported showing that SP binding is highly sensitive to the chirality change of the C-terminal residues (Gln6-Leu10), but less sensitive to the chirality change of the N-terminal residues (Arg1-Gln5). A qualitative analysis of the database by comparison of series of peptide pairs revealed a repeated pattern of affinity change with D-amino acid replacement, suggesting a largely additive binding activity of SP from each residue. On the other hand, possible intramolecular interactions between some N-terminal and C-terminal residues to form an optimal binding conformation were also found. A set of 189 peptides with IC50 values less than 5 microM was subjected to an empirical QSAR analysis using a linear additive model. The relative contribution coefficients obtained agreed with the observation that the predominant contribution comes from the C-terminal residues, suggesting considerable independency of each residue on binding to NK1 receptors.(ABSTRACT TRUNCATED AT 250 WORDS)

P物质类似物的系统研究。2512种结合NK1受体的P物质立体异构体的快速筛选。
多肽合成的最新进展使得同时合成和筛选大量多肽类似物成为可能。我们在这里报告了一个大规模筛选P物质的立体异构体与系统d -氨基酸替代的模型研究。这些研究有助于探索肽-受体相互作用的构象要求,并为肽药物设计提供经验信息。采用多针多肽合成方法制备了512个SP立体异构体。这些类似物的受体结合亲和力通过迭代竞争试验估计。获得的结果形成了SP与中枢NK1受体结合的立体化学要求的综合数据库。单d -氨基酸取代类似物的数据与先前报道的一致,表明SP结合对c端残基(Gln6-Leu10)的手性变化高度敏感,而对n端残基(Arg1-Gln5)的手性变化不太敏感。通过对一系列肽对的比较,对数据库进行定性分析,发现随着d -氨基酸的替换,亲和力发生了重复的变化,这表明每个残基的SP在很大程度上具有加性结合活性。另一方面,还发现了一些n端和c端残基之间可能的分子内相互作用,以形成最佳的结合构象。采用线性加性模型对189个IC50值小于5微米的多肽进行实证QSAR分析。获得的相对贡献系数与观察结果一致,即主要贡献来自c端残基,这表明每个残基与NK1受体的结合具有相当大的独立性。(摘要删节250字)
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